The present invention discloses pharmaceutical-grade ferric organic compounds, including ferric citrate, which are soluble over a wider range of pH, and which have a large active surface area. A manufacturing and quality control process for making a pharmaceutical-grade ferric citrate that consistently complies with the established Manufacture Release Specification is also disclosed. The pharmaceutical-grade ferric organic compounds are suitable for treating disorders characterized by elevated serum phosphate levels.
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1. A method of treating hyperphosphatemia, comprising:
administering one or more tablets comprising ferric citrate and a pharmaceutically acceptable carrier to a subject, the tablets prepared from a form of ferric citrate having a bet active surface area of at least about 16 m2/g;
wherein the tablets are administered to provide up to 30 grams of ferric citrate to the subject per day.
12. A method of treating metabolic acidosis, comprising:
administering one or more tablets comprising ferric citrate and a pharmaceutically acceptable carrier to a subject, the tablets prepared from a form of ferric citrate having a bet active surface area of at least about 16 m2/g;
wherein the tablets are administered to provide up to 30 grams of ferric citrate to the subject per day.
23. A method of treating hyperphosphatemia, comprising:
administering one or more tablets comprising ferric citrate and a pharmaceutically acceptable carrier to a subject, the tablets prepared from a form of ferric citrate having a bet active surface area of at least about 16 m2/g;
wherein the tablets are administered to provide 3 grams to 6 grams of ferric citrate to the subject per day.
30. A method of treating metabolic acidosis, comprising:
administering one or more tablets comprising ferric citrate and a pharmaceutically acceptable carrier to a subject, the tablets prepared from a form of ferric citrate having a bet active surface area of at least about 16 m2/g;
wherein the tablets are administered to provide 3 grams to 6 grams of ferric citrate to the subject per day.
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This application is a Continuation of U.S. Ser. No. 14/306,756, filed Jun. 17, 2014, which is a Continuation of U.S. Ser. No. 13/661,558, filed Oct. 26, 2012, which is a Continuation of U.S. Ser. No. 13/289,048, filed Nov. 4, 2011, which is a Continuation of U.S. Ser. No. 12/064,058, filed Feb. 18, 2008, which is a National Stage of International Application No. PCT/US2006/032385, filed Aug. 18, 2006, which claims the benefit of U.S. Ser. No. 60/709,511, filed Aug. 19, 2005, and is a Continuation-in-part of U.S. Ser. No. 11/206,981, filed Aug. 18, 2005, which is a Continuation-in-part of Int'l App'l No. PCT/US2004/004646, filed Feb. 18, 2004, which claims the benefit of U.S. Ser. No. 60/462,684, filed Apr. 15, 2003, and U.S. Ser. No. 60/447,690, filed Feb. 19, 2003. The entire contents and disclosures of the preceding applications are incorporated herein by reference into this application.
Throughout this application, various publications are referenced. Disclosures of these publications in their entireties are hereby incorporated by reference into this application to more fully describe the state of the art to which this invention pertains.
This invention relates to the preparation and use of pharmaceutical-grade ferric organic compounds, such as ferric citrate. Uses of the pharmaceutical-grade ferric citrate described herein, include, but are not limited to methods of treating various disorders in humans and non-human subjects or patients.
Uses of Iron Compounds
Ferric iron containing compounds are useful in the treatment of a number of disorders, including, but not limited to, hyperphosphatemia and metabolic acidosis. See Hsu et al., “New Phosphate Binding Agents: Ferric Compounds”, J Am Soc Nephrol, Vol. 10, Pages 1274-1280, 1999. Previous studies and inventions have reported the use of ferric compounds in binding with dietary phosphates, and such ferric compounds are potentially useful for the treatment of hyperphosphatemia in renal failure patients (U.S. Pat. No. 5,753,706, 1998; U.S. Pat. No. 6,903,235, 2005; CN 1315174, 2001; Yang W. C., et al., Nephrol. Dial. Transplant 17:265:270 (2002)). Elevated amounts of phosphate in the blood can be removed by administering compounds such as ferric citrate. Once in solution, the ferric iron binds phosphate, and the ferric phosphate compounds precipitate in the gastrointestinal tract, resulting in effective removal of dietary phosphate from the body. It is also believed that the absorbed citrate from ferric citrate is converted to bicarbonate which corrects metabolic acidosis, a condition common in renal failure patients.
Int'l App. No. PCT/US2004/004646, filed Feb. 18, 2004, published under Int'l Publication No. WO2004/074444 on Sep. 2, 2004, discloses a method of preparing ferric organic compounds, including ferric citrate that remains soluble over a wider range of pH than previously described preparations, and which have a large active surface area. However, commercially scalable manufacturing processes with quality control/analysis measures to ensure and/or to verify the compliance of the pharmaceutical-grade ferric citrate or ferric organic compounds with established standards or specifications were not previously disclosed.
Accordingly, there exists a need for a scalable process for synthesizing pharmaceutical-grade ferric organic compounds or ferric citrate for human use. The process needs to consistently produce ferric organic compounds or ferric citrate of the required pharmaceutical grade.
This invention further discloses dosage for ferric citrate for treating of a human or non-human subject or patient in need of the compound. Different routes of administration are explored.
In accordance with these and other objects of the invention, a brief summary of the present invention is presented. Some simplifications and omission may be made in the following summary, which is intended to highlight and introduce some aspects of the present invention, but not to limit its scope. Detailed descriptions of a preferred exemplary embodiment adequate to allow those of ordinary skill in the art to make and use the invention concepts will follow in later sections.
An embodiment of the invention provides a manufacturing and quality control process/analysis for making a pharmaceutical-grade ferric citrate that consistently complies with the established Manufacture Release Specification. The process of the present invention can be adapted to produce multi-kilogram batches of pharmaceutical-grade ferric citrate, and can be readily scaled up to provide additional manufacturing capacity for ferric citrate.
An illustrative embodiment of the manufacturing method may be exemplified by the following non-limiting sequence of steps for preparing pharmaceutical-grade ferric citrate comprising the steps of: (a) dissolving an appropriate amount of Ferric chloride hexahydrate in water to form a Ferric chloride hexahydrate solution; (b) dissolving an appropriate amount of NaOH in water to form a NaOH solution; (c) mixing the Ferric chloride hexahydrate solution and NaOH solution to form a solution with Fe(OH)3 precipitate; (d) maintaining the pH of the solution with Fe(OH)3 precipitate above 7.0; (e) isolating the Fe(OH)3 precipitate; (f) washing the Fe(OH)3 precipitate three times with water; (g) suspending the Fe(OH)3 precipitate in water; (h) adding citric acid to the Fe(OH)3 precipitate to form a ferric-organic acid solution; (i) stirring and heating the ferric-organic acid solution at 90-100° C. for 30 to 120 minutes; (j) removing solids in the ferric-organic acid solution by adding citric acid; (k) allowing the ferric-organic acid solution to cool to below 30° C.; (l) maintaining the pH of the ferric-organic acid solution to between 0.8-1.5; (m) filtering the ferric-organic acid solution to obtain a liquid filtrate; (n) mixing acetone and liquid filtrate to form ferric citrate; (o) isolating ferric citrate; (p) washing ferric citrate with acetone three times; and (q) drying the ferric citrate.
A further embodiment provides a large-scale production scheme for pharmaceutical-grade ferric citrate comprising the steps of: (a) mixing an appropriate amount of NaOH and Ferric chloride hexahydrate in a suitable reactor to form a ferric hydroxide slurry with ferric hydroxide precipitate; (b) maintaining the pH of the ferric hydroxide slurry to above 7.0; (c) isolating the ferric hydroxide precipitate from the ferric hydroxide slurry using pressure filtration; (d) washing the ferric hydroxide precipitate three times; (e) maintaining the % Cl in the ferric hydroxide precipitate to below 5%; (f) isolating the washed ferric hydroxide precipitate using pressure filtration; (g) mixing citric acid with washed ferric hydroxide precipitate to form a ferric organic acid solution; (h) stirring and maintaining the temperature of the ferric organic acid solution at 80±5° C. for 2 hours; (i) allowing the ferric organic acid solution to cool to 60° C.; (j) maintaining the pH of the ferric organic acid solution to between 0.8 to 1.5 and the amount of Fe in the ferric organic acid solution to 85% of Fe added in step (a); (k) filtering the ferric organic acid solution using pressure filtration to obtain a liquid filtrate; (l) mixing the liquid filtrate with acetone to obtain ferric citrate; (m) isolating ferric citrate using pressure filtration; (n) washing the ferric citrate with acetone; (o) isolating the washed ferric citrate using pressure filtration; (p) drying the washed ferric citrate in fluidized bed dryer; and (q) maintaining the organic volatile impurities to ≦1000 ppm acetone.
A further embodiment encompasses various intermediate compositions that may be useful in the preparation of the pharmaceutical-grade ferric citrate. The intermediate compositions encompassed herein include solids, liquids or multiphase mixtures. A liquid intermediate composition comprising the pharmaceutical-grade ferric citrate may be an aqueous composition or an organic solvent-based composition. A multiphase composition may encompass both aqueous and organic phases.
An additional embodiment encompasses the methods of storing, packaging and using the various intermediate compositions disclosed herein.
An additional embodiment provides pharmaceutically useful compositions comprising the pharmaceutical-grade ferric citrate. The pharmaceutically useful composition further comprises any pharmaceutically acceptable carrier, adjuvant, filler or delivery vehicle suitable for administering to a subject or human patient, an effective amount of the pharmaceutical-grade ferric citrate.
Further embodiments of the pharmaceutical compositions include, but are not limited to solids, liquids, or semi-solid forms, such as gels, syrups, chewables or pastes.
Within the scope of the methods of using the pharmaceutically useful compositions disclosed herein are effective doses of the pharmaceutical compositions, in addition to the timing and modes of administering the pharmaceutical compositions.
A non-limiting example of a method for using the pharmaceutical compositions encompasses treating disorders resulting from elevated blood levels of phosphates, i.e., hyperphosphateimia, in a subject or a human patient. Such disorders are exemplified by, but not limited to, renal failure or the progression of renal failure, mineralization of soft tissues, hyperparathyroidism as well as other complications.
An embodiment encompassed by the invention includes a pharmaceutical composition comprising:
The pharmaceutical composition described herein may be prepared by a method shown in
An additional embodiment encompasses compositions of pharmaceutical-grade ferric citrate, prepared according to methods comprising the steps of:
It is advantageous to scale-up the method of preparation. Thus, an industrial-scale method is embodied by a method for large-scale production of pharmaceutical-grade ferric citrate comprising the steps of:
The compositions encompassing pharmaceutical grade ferric citrate are suitable for treating hyperphosphatemia, or other disorders characterized by high serum phosphate levels. Therefore, the invention encompasses treating subjects or patients with various renal diseases; e.g., End Stage Renal Diseases (ESRD), Chronic Kidney Disease (CKD) or other relate kidney diseases, or subjects and patients who are on dialysis but not limited to hemodialysis.
In another embodiment, the compositions encompassing pharmaceutical grade ferric citrate may used to treat subjects or patients with metabolic acidosis. Other disorders that may be ameliorated by the conversion of citrate to bicarbonate are also encompassed by the invention described.
An embodiment of a method for using the pharmaceutical composition encompasses treating a human or non-human subject or patient with chronic kidney disease. There are generally five clinical stages of chronic kidney disease, numbered 1 to 5, wherein stage 1 is the least severe and stage 5 the most severe. In the early stages, e.g., stages 1 and 2, dialysis is not required. As chronic kidney disease progresses to stage 5, a patient may require dialysis treatment three times per week. It should be noted that elevated phosphate levels are observed at all stages of chronic kidney disease. Therefore, an embodiment of the invention is a method of treating a subject or person with early or mid-stage chronic kidney disease, with a composition comprising pharmaceutical-grade ferric citrate in order to achieve a lower serum phosphate level.
It is a further embodiment of the invention to provide a method of treating a human or non-human subject or patient with late-stage chronic kidney disease who undergo hemodialysis, by administering a composition comprising pharmaceutical-grade ferric citrate. It is known that hemodialysis is not sufficiently effective in reducing serum phosphate level. The treatment of a subject or person with late stage kidney disease is applicable whether or not the subject or person is currently undergoing hemodialysis treatment.
An additional embodiment of the invention is a method of treating a subject or person with chronic kidney disease and undergoing peritoneal dialysis with the pharmaceutical-grade ferric citrate-containing compositions described. It is known that peritoneal dialysis is not sufficiently effective in reducing serum phosphate levels.
An additional embodiment is a method for using the pharmaceutical composition to inhibit or even reverse soft tissue mineralization, specifically calcification. Hyperphosphatemia may lead to increased calcium phosphate deposition in hard and soft tissues by increasing the likelihood of binding with free calcium to form insoluble calcium phosphate. Therefore, an effective dose of a composition comprising pharmaceutical-grade ferric citrate may decrease serum phosphate levels and result in a corresponding decrease in calcium phosphate deposition.
It is noteworthy that whereas ferric ion forms insoluble precipitates with phosphate-containing compounds in the lumen of the gastroinstestinal tract, the citrate component is absorbed and functions as a calcium chelator. Because chelated calcium is not available for calcium phosphate formation, administering pharmaceutical-grade ferric citrate decreases may lead to reductions in both serum calcium and phosphate. This may also be expressed as leading to a decrease in the serum calcium-phosphate product. Reducing serum calcium and phosphate would be expected to reduce calcium phosphate deposition. The end result is reversing, i.e., solubilizing or dissolving, the deposited calcium phosphate.
The decalcifying of a calcified soft tissue, e.g., the sclera of the eye, may be achieved by administering pharmaceutical-grade ferric citrate. It is known among persons of ordinary skill in the relevant medical arts that patients with kidney disease receiving doses of ferric citrate have shown reversal of calcium deposits on the eye. Therefore, an embodiment of the invention is directed to the decalcification of soft tissue such as the eye.
Kidney stones comprise calcium salts of oxalic acid or phosphates and are formed by mechanisms similar to those described above. Thus, pharmaceutical-grade ferric citrate, in another embodiment of the invention provides a method of treating kidney stones, i.e., renal calculi, by promoting their dissolution.
The compositions encompassing pharmaceutical grade ferric citrate may operate according to more than one mechanism. A plausible non-limiting mechanism of action may result from the ferric ion binding phosphate in the GI tract, thus forming an insoluble ferric phosphate precipitate. This, in turn, may result in decrease the uptake of phosphate and phosphate-containing compounds from the GI tract.
In view of such a mechanism, the administering of compositions encompassing pharmaceutical grade ferric citrate via an oral route is encompassed by the inventive methods described.
This invention provides a method of reversing, preventing or stabilizing soft tissue calcification of a subject, comprising administering to said subject and effective amount of a ferric citrate compound.
This invention further provides a method of reversing, preventing or stabilizing soft tissue calcification of a subject, comprising administering to said subject and effective amount of a ferric citrate compound, wherein the ferric citrate compound is prepared according to a method as shown in
This invention provides a method of reversing, preventing or stabilizing soft tissue calcification of a subject, comprising administering to said subject and effective amount of a ferric citrate compound, wherein the ferric citrate compound is prepared according a method comprising the steps of:
An embodiment of the invention encompasses tolerable doses of up to 15 grams per day for ferric citrate capsules and 30 grams per day for ferric citrate tablets.
The compositions encompassing pharmaceutical grade ferric citrate may be administered for varying periods of time. In some embodiments, the tolerability of the compositions encompassing pharmaceutical grade ferric citrate allows for long term administration when necessary.
In drawings which illustrate specific embodiments of the invention, but which should not be construed as restricting the spirit or scope of the invention in any way:
In drawings which illustrate specific embodiments of the invention, but which should not be construed as restricting the spirit or described in detail to avoid unnecessarily obscuring the invention. Accordingly, the specification and drawings are to be regarded in an illustrative, rather than a restrictive, sense.
Throughout this application, references are made to the United States Pharmacopeia (USP), and the latest edition of the USP, USP 28, is hereby incorporated by reference into this application in its entirety.
This invention provides a method of preparing pharmaceutical-grade ferric citrate, comprising the steps of: (a) dissolving an appropriate amount of Ferric chloride hexahydrate in water to form a Ferric chloride hexahydrate solution; (b) dissolving an appropriate amount of NaOH in water to form a NaOH solution; (c) mixing the Ferric chloride hexahydrate solution and NaOH solution to form a solution with Fe(OH)3 precipitate; (d) maintaining the pH of the solution with Fe(OH)3 precipitate above 7.0; (e) isolating the Fe(OH)3 precipitate; (f) washing the Fe(OH)3 precipitate three times with water; (g) suspending the Fe(OH)3 precipitate in water; (h) adding citric acid to the Fe(OH)3 precipitate to form a ferric-organic acid solution; (i) stirring and heating the ferric-organic acid solution at 90-100° C. for 30 to 120 minutes; (j) removing solids in the ferric-organic acid solution by adding citric acid; (k) allowing the ferric-organic acid solution to cool to below 30° C.; (l) maintaining the pH of the ferric-organic acid solution to between 0.8-1.5; (m) filtering the ferric-organic acid solution to obtain a liquid filtrate; (n) mixing acetone and liquid filtrate to form ferric citrate; (o) isolating ferric citrate; (p) washing ferric citrate with acetone three times; and (q) drying the ferric citrate.
This invention provides a method for scalable or large-scale production of pharmaceutical-grade ferric citrate comprising the steps of: (a) mixing an appropriate amount of NaOH and Ferric chloride hexahydrate in a suitable reactor to form a ferric hydroxide slurry with ferric hydroxide precipitate; (b) maintaining the pH of the ferric hydroxide slurry to above 7.0; (c) isolating the ferric hydroxide precipitate from the ferric hydroxide slurry using pressure filtration; (d) washing the ferric hydroxide precipitate three times; (e) maintaining the % Cl in the ferric hydroxide precipitate to below 5%; (f) isolating the washed ferric hydroxide precipitate using pressure filtration; (g) mixing citric acid with washed ferric hydroxide precipitate to form a ferric organic acid solution; (h) stirring and maintaining the temperature of the ferric organic acid solution at 80±5° C. for 2 hours; (i) allowing the ferric organic acid solution to cool to 60° C.; (j) maintaining the pH of the ferric organic acid solution to between 0.8 to 1.5 and the amount of Fe in the ferric organic acid solution to ≧85% of Fe added in step (a); (k) filtering the ferric organic acid solution using pressure filtration to obtain a liquid filtrate; (l) mixing the liquid filtrate with acetone to obtain ferric citrate; (m) isolating ferric citrate using pressure filtration; (n) washing the ferric citrate with acetone; (o) isolating the washed ferric citrate using pressure filtration; (p) drying the washed ferric citrate in fluidized bed dryer; and (q) maintaining the organic volatile impurities to ≦1000 ppm acetone.
In an embodiment, the ferric chloride hexahydrate complies with the release specification as shown in Table B; the citric acid complies with the release specification as shown in Table F; the water complies with the release specification as shown in Table D; the acetone complies with the release specification as shown in Table E; and the sodium hydroxide complies with the release specification as shown in Table C.
In another embodiment, the ferric citrate is dried using a fluidized bed dryer or is dried under vacuum.
In a further embodiment, the process as described above further comprises testing the ferric citrate for compliance with the release specification as shown in Table A. In a further embodiment, testing comprises performing at least one test selected from the group consisting of: assay content purity of ferric citrate and ferric citrate monohydrate; assay content of citric acid; assay content of detectable ferric citrate related substances; assay content of ferric ion; elemental iron impurity test; limit of ferrous iron test; loss on drying test; hydrate test (water content by differential scanning calorimetry); hydrate test (water content by karl Fischer Titration); trace or heavy metals test (As, Ca, Cd, Cu, Fe, Hg, Na, Pb, Sr, Zn); limit of oxalic acid test; identification A for ferric salts test; identification B by FTIR test; insoluble substances test; limit of ammonium test; limit of chloride test; limit of nitrate test; limit of tartrate test; residue on ignition test; organic volatile impurities test; and microbial, mold and yeast test.
This invention provides a pharmaceutical-grade ferric citrate prepared according to the methods described above.
This invention provides a composition comprising the ferric citrate prepared according to the methods described above for treating hyperphosphatemia or metabolic acidosis.
This invention provides a composition prepared according to the methods described above for treating disorders responsive to ferric organic compound therapy.
This invention provides a pharmaceutical-grade ferric citrate prepared according to the methods described above, wherein the ferric citrate produces the peak as shown in
This invention provides a pharmaceutical-grade ferric citrate prepared according to the methods described above, wherein the ferric citrate possesses the dissolution rates as shown in
This invention provides a pharmaceutical-grade ferric citrate prepared according to the methods described above, wherein the ferric citrate produces the spectral data as shown in
This invention provides a composition comprising the ferric citrate as described above for treating hyperphosphatemia or metabolic acidosis.
This invention provides a composition comprising the ferric acid as describe above for treating disorders responsive to ferric organic compound therapy.
This invention provides a pharmaceutical-grade ferric citrate prepared by the process comprising the steps as shown in
The pharmaceutical-grade ferric citrate according to the invention is useful for treating a subject suffering from hyperphosphatemia, metabolic acidosis or a disorder responsive to ferric organic compound therapy. In an embodiment, the subject is a human being.
The invention also provide a use for a composition comprising pharmaceutical-grade ferric citrate effective for one or more of the following uses,
The use may further encompass at least partly relying on reducing serum levels of calcium and phosphate ions.
The uses as stated above may apply to soft tissue such as a blood vessel or an eye.
The uses as stated may be carried out by administering over a long-term.
The invention allows for the above-stated uses to be achieved wherein the use is accompanied by less gastronintestinal adverse side effects than if the composition comprised chemical grade ferric citrate.
In accordance with the above-stated uses, the invention provides for a method for treating a disorder characterized by a high serum phosphate level comprising administering an effective amount of a composition comprising pharmaceutical-grade ferric citrate.
The invention also provides for the method wherein an effective amount of pharmaceutical-grade ferric citrate is administered in the form of a tablet, a powder, a suspension, an emulsion, a capsule, a lozenge, a granule, a troche, a pill, a liquid, a spirit, or a syrup.
The invention also provides for the method wherein the effective amount of pharmaceutical-grade ferric citrate is from 2 to 100 grams per day, preferably between 4 and 60 grams per day.
In some embodiments, the method may provide a daily effective amount of 2, 4, 6, or 8 grams.
In general, hyperphosphatemia is prevalent in patients with chronic renal failure and in patients on dialysis. There is also evidence that indicate elevated serum phosphorus, calcium-phosphorus product (Ca×P) and parathyroid hormone (PTH) levels contribute to increased incidence of vascular, visceral, peripheral vascular and soft tissue calcification in renal disease patients
Thus, it is an additional novel feature of the claimed invention to prevent or reverse calcification in renal disease patient or in a normal person. For example, dissolving kidney stones that may accompany renal failure.
Phosphorous exerts a negative impact on vascular calcification by direct participation in the Ca×P and indirectly in the pathogenesis and progression of hyperthyroidism. Serum calcium and phosphorous are metastable under normal circumstances, which means that their concentrations are not sufficient to produce spontaneous precipitation. However, once the calcification process begins, the concentrations are sufficient to support crystal proliferation.
Available evidence confirms a high prevalence of underlying vascular disease and structural heart disease in patients with severe chronic renal failure. These structural lesions are then exposed to elevated serum phosphorus, Ca×P, and PTH(1).
Factors which are considered likely to contribute to elevated serum phosphorus and Ca×P include administration of calcium-containing phosphorus binders. The calcium-containing phosphorus binders, such as calcium acetate are prescribed to many new hemodialysis (HD) and peritoneal dialysis (PD) patients, thus providing a large source of exogenous calcium to the GI tract.
Calcification also extends beyond renal disease patients and can include anyone who is over the age of 40. While the leading cause of death in the United States is acute myocardial infarction and stroke, hypercholesteromia contribute to only 15% of the deaths in this category and 85% is caused by ventricular calcification.
It has been shown that abnormalities in serum phosphorous, Ca×P and PTH levels can result in vascular, visceral and/or soft tissue calcification. For example, calcifications of myocardium, coronary arteries, cornea can lead to the development of a number of clinically significant complications including myocardial ischemia, myocardial infarction, impaired myocardial function, congestive heart failure, cardiac valve insufficiency and blindness.
Accordingly, there exists a need for methods of managing or reducing serum phosphorous as a means of treating numerous medical disorders. The method includes administering a phosphate binder which does not adversely affect serum calcium levels and does not cause toxic side effects in the patient.
In examples which are intended to illustrate embodiments of the invention but which are not intended to limit the scope of the invention:
Referring to
Examples of quality control measures employed in the synthesis process include: (QC4) maintaining pH of the ferric hydroxide slurry above 7.0; (QC5) maintaining the % Cl in ferric hydroxide precipitate below 5%; (QC7) maintaining the pH of the mixture between 0.8-1.5 and the Fe in mixture ≧85% of total Fe added after adding citric acid to ferric hydroxide precipitate; and (QC9) maintaining the level of acetone to ≦1000 ppm during the drying stage.
In an embodiment, the raw materials, i.e., ferric chloride, deionized water, citric acid, acetone, sodium hydroxide, must pass release specifications, such as those provided on Table B-F, before they can be used in the synthesis process. See
Referring to
Examples of quality control measures employed in the synthesis process include: (QC4A) maintaining pH of the ferric hydroxide slurry above 7.0; (QC5A) maintaining the % Cl in ferric hydroxide precipitate below 5%; (QC7A) maintaining the pH of the mixture between 0.8-1.5 and the Fe in mixture ≧85% of total Fe added after adding organic acid to ferric hydroxide precipitate; and (QC9A) maintaining the level of organic solvent to ≦1000 ppm during the drying stage.
In an embodiment, the raw materials, i.e., ferric iron salt, deionized water, organic acid, organic solvent, alkaline metal hydroxide, must pass release specifications before they can be used in the synthesis process. See
The ferric organic compounds produced according to the methods described above are more soluble than commercially available ferric organic compounds, over a wider range of pH levels. This increase in solubility of the ferric organic compounds of the present invention is believed to be a result of the unique significantly large active surface area of the ferric organic compounds of the present invention. For example, at pH 8.0, the intrinsic dissolution rate of ferric citrate of the present invention is 3.08 times greater than the commercially available ferric citrate. See Table 1.
The intrinsic dissolution rates of commercially available ferric citrate were compared with the ferric citrate of the present invention. The intrinsic dissolution rate is defined as the dissolution rate of pure substances under the condition of constant surface area. The dissolution rate and bioavailability of a drug substance is influence by its solid state properties: crystallinity, amorphism, polymorphism, hydration, solvation, particle size and particle surface area. The measured intrinsic dissolution rate is dependent on these solid-state properties and is typically determined by exposing a constant surface area of a material to an appropriate dissolution medium while maintaining constant temperature, stirring rate, and pH. The intrinsic dissolution rates are presented in Table 1.
TABLE 1
Intrinsic dissolution rates of ferric
citrate at 37° C. in solutions of pH 8
Mean
Rate of
Intrinsic
Intrinsic
Acetone
Dissolution
Dissolution
Addition
Rates
Rates
Sample
(ml/min)
(mg/cm2/min )
(mg/cm2/min)
RFS-12 (sigma/
10.0
0.83
0.83
commercially
available)
STM-134
10.0
1.88
3.08
(reference
material)
PAN031203A
10.0
3.82
(experimental
batch 1)
PAN031203B
10.0
4.00
(experimental
batch 2)
PAN031203C
9.5
2.68
(experimental
batch 3)
PAN031203D
40
2.95
(experimental
batch 4)
PAN031203E
4.4
3.13
(experimental
batch 5)
For example, the BET active surface area of the ferric citrate of the present invention is at least 16 times larger than the commercially available ferric citrate. See Table 2.
The analysis of active surface area is based on BET theory which describes the phenomenon of mass and energy interaction and phase changes during gas adsorption onto solid surfaces and in pore spaces. In BET active surface area measurement, the volume of a monolayer of gas is determined which allows the surface area of the sample to be determined using the area occupied by a single layer of adsorbed gas molecule. Table 4 is a comparison of the active surface area of the ferric citrate of the present invention compared to the active surface area of commercially available ferric citrate compounds.
TABLE 2
BET active surface areas of various forms of ferric citrate
Mean Dissolution
BET Active
Rates
Surface
Sample
(mg/cm2/min)
Area
RFS-12-1 (sigma/commercially
0.76
0.61
available)
RFS-12-2 (sigma/commercially
available)
STM-134-1 (reference material 1)
2.47
16.17
STM-134-2 (reference material 2)
STM-182-1 (lab-scale 500 g batch 1)
2.61
19.85
STM-182-2 (lab-scale 500 g batch 2)
The ferric organic compounds produced according to the methods described above are useful in the treatment of hyperphosphatemia, metabolic acidosis, and any other disorders responsive to ferric organic compound therapy. Because the ferric organic compounds of the present invention are more soluble than commercially available ferric organic compounds, smaller amounts of the ferric organic compounds of the present invention can be used to effectively treat patients suffering from such disorders.
Improved aqueous solubility is particularly relevant to the use of the ferric organic compounds of the present invention in the treatment of disorders responsive to ferric organic compound therapy. Because the ferric organic compounds of the present invention are more soluble, they will be more effective when taken orally, and therefore can be taken in lower doses. The ferric organic compounds of the present invention are more soluble over a wider pH range than commercially available ferric organic compounds; therefore, the ferric organic compounds of the present invention can be more effective by being soluble in the small intestine.
For example, in an experiment simulating the alkaline condition in the small intestine, the ferric citrate of the present invention showed better dissolution rate than the commercially available ferric citrate. It is suggested that the ferric citrate of the present invention can be more effective by being more soluble in the small intestine. See Table 1. As a result, patients can take lower doses of medication with lower incidences of side effects.
In one embodiment of the invention, the ferric citrate of the present invention has a significantly higher rate of aqueous solubility under physiological conditions than commercially available forms of ferric citrate, and therefore the ferric citrate of the present invention is believed to provide a significant improvement in the orally effective use of ferric citrate at a reduced dosage. By reducing the orally effective dose of ferric citrate, it is believed that the ferric citrate of the present invention will provide a lower incidence of ulcerative gastrointestinal adverse effects associated with commercially available ferric citrate compounds. In addition, it is believed that the increased rate of dissolution of the ferric citrate of the present invention will provide a more rapid onset of action in binding to dietary phosphate.
The ferric organic compounds of the present invention can be administered in a number of forms, including orally administrable forms, which can comprise the ferric organic compounds of the present invention alone or in combination with a pharmaceutically acceptable carrier. The orally administrable form includes, but is not limited to, a tablet, a powder, a suspension, an emulsion, a capsule, a granule, a troche, a pill, a liquid, a spirit, or a syrup. The composition can be administered to human beings or other animals suffering from illnesses responsive to ferric organic compound therapy.
The present invention describes a process for manufacturing pharmaceutical-grade ferric citrate suitable as an active pharmaceutical ingredient for human use. An overview of the Ferric Citrate Manufacture Flow Chart is shown in
4.1. Preparation of Ferric Chloride Solution
Weigh 550 g of ferric chloride hexahydrate (correct for CoA purity) into a 1 L beaker.
Transfer the ferric chloride hexahydrate into a 4 L Erlenmeyer flask.
Measure 1.1 L of deionized water using a graduated cylinder. Use a small portion of the deionized water to rinse the beaker and transfer the water into the 4 L Erlenmeyer flask. Transfer the remaining water into the Erlenmeyer flask.
Stir solution using a magnetic stirring bar until completely dissolved. The solution is a dark yellow to dark brown color.
4.2. Preparation of Sodium Hydroxide Solution
Weigh 244 g of sodium hydroxide (correct for CoA purity) into a 500 mL beaker.
Transfer the sodium hydroxide into a 2 L Erlenmeyer flask.
Measure 1.1 L of deionized water using a graduated cylinder. Use a small portion of the deionized water to rinse the beaker and transfer the water into a 4 L Erlenmeyer flask. Transfer the remaining water into the Erlenmeyer flask slowly.
In a fumehood, stir the solution using a stirring bar while adding the water and stir until completely dissolved. The solution is clear and colorless.
Cool solution to below 30° C. using a water bath.
4.3. Preparation of Ferric Hydroxide Intermediate
Place a magnetic stirring bar into the ferric chloride solution and place the flask in a water bath. Set up on a stirring plate and start the stirring plate at a low speed.
Add slowly the sodium hydroxide solution to the ferric chloride solution (at a rate of less than 20 mL/min) using an addition funnel and control the temperature of the reaction mixture below 40° C. using the water bath and the rate of addition of sodium hydroxide.
Continue to cool the brown viscous mixture to below 30° C. using the water bath.
The final pH should be above 7. Use a suitable volume of 5 M aqueous sodium hydroxide solution to correct the pH if not above 7. Measure and record the final pH. A dark brown precipitate of ferric hydroxide is formed.
If required, cool the brown viscous mixture to below 30° C. using the cold water bath and filter the ferric hydroxide suspension through 1 mm size stainless steel filter to break up large precipitates.
Transfer equal amounts of ferric hydroxide suspension into four 500 mL centrifuge containers. Balance the weight of each centrifuge container using a top-loading balance before centrifugation.
Centrifuge the ferric hydroxide suspension at 1500 rpm and 25±5° C. for 5 minutes. Discard the supernatant.
Measure 2.5 L of deionized water using a graduated cylinder and use approximately 1 L of water to re-suspend the ferric hydroxide precipitate from the centrifuge containers.
Transfer the ferric hydroxide suspension into a 4 L Erlenmeyer flask fitted with a 1 mm size stainless steel filter over a glass funnel. Use the remaining 1.5 L of deionized water to rinse the containers and wash the precipitate retained on the stainless steel filter.
Wash the precipitate two more times by repeating the steps beginning with “Transfer equal amounts . . . ”
After the third wash, recover the precipitate by repeating the steps beginning with “Transfer equal amounts . . . ” and ending with “Centrifuge the ferric hydroxide suspension . . . ”
Re-suspend the precipitate in 150 mL of deionized water.
4.4. Preparation of Ferric Citrate
Homogenize the ferric hydroxide precipitate using a mechanical stirrer for 5 min in a 2 L Erlenmeyer flask.
Weigh 490 g of citric acid (correct for CoA purity) into a 500 mL beaker.
Place a stir bar in the 2 L Erlenmeyer flask in an oil bath and stir at high speed.
Add the citric acid into the ferric hydroxide suspension.
Stir the solution for 30 minutes.
Heat the mixture at 90 to 100° C. (in oil bath) until the color changes from orange-brown to a clear black-brown (for 30 to 120 min) or until ferric hydroxide precipitate is dissolved.
Take 1 mL aliquot of the reaction mixture in a 6 mL glass test tube and centrifuge at 1500 rpm and 25±5° C. for 5 minutes. Proceed to the next step if no precipitate is observed. If some precipitate is observed add 10 to 34 g citric acid to the mixture and continue heating for 10 to 30 min.
Terminate the heating and cool the mixture to below 30° C. Measure the pH of the reaction mixture; it should be pH 0.8 to 1.5.
Transfer equal amounts of the reaction mixture into four 500 mL centrifuge containers and balance the weight of each container using a top-loading balance.
Centrifuge the reaction mixture at 1500 rpm and 25±5° C. for 5 minutes. Transfer and pool all the ferric citrate supernatant to a clean 4 L Erlenmeyer flask.
Repeat the above 2 steps for all of the ferric citrate reaction mixture.
Place one-half of the ferric citrate supernatant in a 4 L Erlenmeyer flask and stir with a magnetic stir bar at high speed.
Add slowly (over 20 min) 3.5 L of acetone (accurate volume acetone calculated as five fold the supernatant volume) and stir for an additional 10 min. A light-beige color precipitate forms.
Transfer the suspension into four 500 mL centrifuge containers and balance the weight of each container using a top-loading balance.
Centrifuge the ferric citrate suspension at 1500 rpm and 25±5° C. for 5 minutes.
Transfer and pool all the ferric citrate precipitate to a clean 4 L Erlenmeyer flask.
Repeat the above 4 steps with the second half of the ferric citrate supernatant.
Pool all ferric citrate precipitate, add 1.4 L of acetone and stir for 5 min.
Transfer the suspension into four 500 mL centrifuge containers and balance the weight of each container using a top-loading balance.
Centrifuge the suspension at 1500 rpm and 25±5° C. for 5 minutes.
Repeat the above 2 steps until all suspension is centrifuged.
Transfer and pool all the ferric citrate precipitate to a clean 4 L Erlenmeyer flask.
Repeat the above 5 steps two additional times (total of 3 washes).
Label and weigh drying trays, and record their weight.
Transfer the ferric citrate precipitate onto the drying dishes and dry at ambient temperature (25±5° C.) for 16 hours.
Place the drying trays with precipitate into a vacuum oven and dry at ambient temperature (25±5° C.) and under vacuum (about 20 mm Hg) for 8 to 16 hours (until the material appears ready for grinding).
Reduce the particle size of the ferric citrate in a porcelain mortar and pestle.
Place the ferric citrate powder into a vacuum oven and dry at ambient temperature (25±5° C.) and under vacuum (about 20 mm Hg) for 8 to 24 hours, until the material appears ready for sieving.
Finely reduce the ferric citrate particle size in a porcelain mortar and pestle. Screen the ferric citrate powder through a 45 mesh size (355 micron) sieve.
Transfer the ferric citrate powder into drying trays and place the trays in an oven to dry at 25±5° C. and under high vacuum until the material appears dry (20 to 48 hours).
Transfer the powder into pre-weighed plastic amber containers.
Label and store the containers at ambient temperature and protected from light.
The present invention provides a scalable manufacturing of pharmaceutical-grade ferric citrate. Preferably, the ferric citrate manufacturing process is capable of producing at least 125 kg batches of pharmaceutical-grade ferric citrate. An overview of the ferric citrate manufacturing is shown in
The scalable manufacturing process further employs fluidized bed dryer for drying wet ferric citrate and for attaining release specifications for organic volatile impurities. See Table A for the Manufacture Release Specifications for Pharmaceutical-Grade Ferric Citrate.
This invention provides a pharmaceutical-grade ferric citrate which complies with the Manufacture Release Specifications as shown below in Table A. The pharmaceutical-grade ferric citrate of consistent purity and quality can be prepared using the manufacturing process of the present invention. See
TABLE A
Manufacture Release Specification for Pharmaceutical-Grade Ferric Citrate
Test Item
Method
Limit of Specification
Appearance
Visual
Light brown to beige
powder
Purity of solid state ferric
Calculate based on LC/MS - flow
NLT 90% w/w
citrate
injection quantitation and profile,
anhydrous basis
based on USP 25 <621>, <731>,
<1086>, <736>
Assay content of ferric
LC/MS - flow injection profile,
Run and report as %
citrate non-related
based on USP 25 <621>, <731>,
w/w anhydrous basis
substances in solution state
<1086>, <736>
(attach table summary)
Assay content purity of
LC/MS - flow injection
NLT 70% w/w
ferric citrate and water
quantitation, based on USP 25
anhydrous basis
adduct in solution state
<621>, <731>, <1086>, <736>
Assay content of citric acid
LC/MS - flow injection
NLT 10% w/w
related substance in
quantitation, based on USP 25
anhydrous basis
solution state
<621>, <731>, <1086>, <736>
Assay content of other
LC/MS - flow injection profile,
Run and report as %
ferric citrate related
based on USP 25 <621>, <731>,
w/w anhydrous basis
substances in solution state
<1086>, <736>
(attach table summary)
(excluding citric acid)
Assay content of ferric iron
Based on USP 25 ferric sulfate
NLT 16% w/w fresh
assay
weight basis
Limit of ferrous iron
Gravimetric method using
NMT 1% w/w fresh
potassium ferricynide, based on
weight basis
USP 25 <191>
Loss on drying
USP 25 <731>
NMT 20%
Hydrate (water content)
Karl Fischer Titration
NMT 20%
USP 25 <921> water
determination, Method Ia (Direct
Titration)
Identification
Method A: based on USP 25
Dark blue precipitate
<191> ferric salt
with K4Fe(CN)6 TS;
reddish brown ppt with
excess 1N NaOH;
deep red color not
destroyed by mineral
acids with NH4SCN TS
Sample solution gives
light red color with
pyridine and acetic
anhydride
Limit of chloride
Based on USP 25 Ferric sulfate
NMT 5%
procedures
Reside on ignition
Modified USP 25 <281>
Run and report
Organic Volatile
Based on USP 25 <467>
Acetone not more than
Impurities
1000 ppm
Limit of acid insoluble
Gravimetric determination, based
Not more than 0.02%
substances
on USP 25, ferric sulfate
w/w fresh weight basis
Trace/heavy metals
USP 25 method <231> or
As < 0.3 ppm
equivalent
Others: run and report
ICP for Zn, Cu, Sr, Ca, Na
GFAAS for As
Lead, Cadmium
ICP-MS
Pb < 5 ppm
Cd < 2 ppm
Mercury
Cold vapor/AA
Hg < 0.3 ppm
Total iron content
ICP
NLT 16% w/w fresh weight basis
Microbial/Mold and
USP Method <61>
Yeast
Salmonella
Salmonella = negative
E. Coli
E. Coli = negative
Coliforms
Total Coliforms < 3 cfu/g
Total aerobic count
Total aerobic count < 10 cfu/g
Total combined mold and yeast
Total mold and yeast < 20 cfu/g
TABLE B
Ferric chloride hexahydrate Release Specifications
Test Item
Method
Limit of Specification
Appearance
Visual
Yellow to yellowish brown powder,
crystals or chunks
Identification -
USP 25 <191>
Yield dark blue precipitate with
Ferric salts
potassium ferrocyanide TS
Form reddish brown precipitate with
excess 1N NaOH
Red deep color with ammonium
thiocyanate TS and color not
destroyed by dilute mineral acids
Identification -
USP 25 <191>
Aqueous solution of ferric chloride
Chloride
yields with 0.1N silver nitrate TS
a white, cruddy precipitate, which
is insoluble in nitric acid but is
soluble in a slight excess of 6N
ammonium hydroxide
Heavy metals
ICP-MS
As < 0.1 ppm
Cd < 0.1 ppm
Hg < 0.1 ppm
Pb < 0.1 ppm
Assay - Ferric
USP 25, Assay
>18%
iron
ferric sulfate,
p. 2303
TABLE C
Sodium Hydroxide Release Specifications
Test Item
Method
Limit of Specification
Appearance
Visual
White pellets, odorless
Identification -
USP25, <191>
No precipitate is formed with
Sodium
potassium carbonate
A dense precipitate is formed
with potassium pyroantimonate
An intense yellow color to a non-
luminous flame
TABLE D
Deionized Water Release Specification
Test Item
Method
Limit of Specification
Appearance
Visual
Clear, colorless and odorless
Mineral scan
ICP-MS
As < 0.001 ml/L
Cd < 0.0002 ml/L
Pb < 0.001 ml/L
Hg < 0.02 μg/L
Total Organic
Standard
<1 mg/L
Carbon
Method for the
Examination
of Water and
Wastewater,
20th ed.
Total Hardness
Standard
<4 mg/L
Method for the
Examination
of Water and
Wastewater,
20th ed.
Total Plate
USP 25 method
<10 cfu
Count
<61>
Total Coliform
USP 25 method
<3 cfu
Count
<61>
TABLE E
Acetone Release Specification
Test Item
Method
Limit of Specification
Appearance
Visual
Clear colorless liquid
Identification -
USP 25,
The IR absorption of a thin film
Acetone
p. 2502, FTIR
between KBr plates exhibits a
strong band at about 5.8 μm; a
strong region of absorption
between 6.8 and 7.5 μm, with
maxima at about 7.0 and 7.3 μm;
a strong maximum at about 8.2
μm; and a weak maxima at about
9.2 and 11.0 μm.
Assay
From
NLT 99.5%
manufacturer's
Certificate
of Analysis
(result from
GC method
preferred)
Aldehyde
From
NMT 0.002%
(as HCHO)
manufacturer's
Certificate
of Analysis
Isopropyl
From
NMT 0.05%
alcohol
manufacturer's
Certificate
of Analysis
Methanol
From
NMT 0.05%
manufacturer's
Certificate
of Analysis
Residue after
From
NMT 5 ppm
evaporation
manufacturer's
Certificate
of Analysis
Acids
From
NMT 0.0003 meq
manufacturer's
Certificate
of Analysis
(result from
titrimetric
test)
Bases
From
NMT 0.0006 meq
manufacturer's
Certificate
of Analysis
(result from
titrimetric
test)
Water
From
NMT 2%
manufacturer's
Certificate
of Analysis
Insoluble
From
filtered through ≦0.45 μm filter
substances
manufacturer's
Certificate
of Analysis
or filtered
through ≦0.45
μm filter
TABLE F
Citric Acid Release Specification
Test Item
Method
Limit of Specification
Appearance
Visual
White or colorless crystals or
powder
Identification -
USP 25 <191>
A light red color is produced
Citrate
The following tests are performed to ensure the final ferric citrate product prepared according to the method or process of the present invention complies with the established Manufacture Release Specification as shown in Table A. The Manufacture Release Specification may be readily modified or revised by one of ordinary skill in the art following the teaching of this invention to enhance the purity and safety of the pharmaceutical-grade ferric citrate for human use.
A. Handling and Forms of Test Compositions
Ferric Citrate is Supplied in 500 mg Capsules, whereas the placebo will be provided in identical-looking capsules (indistinguishable from those containing the active drug); the placebo capsules will contain sorbitol and colorant to match the powder color of the active capsules. The placebo capsule shells will be identical to the active capsule shells.
Storage
All study drug supplies must be stored under secure conditions and are not to be used after their expiration date, which is imprinted on the study drug container. The study drugs should be kept under controlled conditions (15 to 30° C.; 59 to 86° F.) in a tightly closed container, protected from light.
Dosage
A recent pilot study compared ferric citrate (3 g daily) to calcium carbonate (3 g daily) for reducing serum PO4 in patients with End Stage Renal Disease (ESRD). Although ferric citrate caused a significant decrease in serum P04, it was not as effective as calcium carbonate. This dose of ferric citrate was associated with mild, but tolerable GI symptoms.
As shown in
The doses of ferric citrate chosen for study or treatment may be from 1 to 30 grams of ferric citrate per day. In part, this may depend on the nature of the formulation provided. For example, ferric citrate capsules may be administered up to a daily dose of about 15 grams/day, whereas the tablet form may be administered up to 30 grams/day. Thus, there is a very broad range of dosing regimens encompassed by the invention.
Titration of Optimal Dosage for a Subject
In the context of this invention, the term “subject” refers to either a human or non-human animal.
The optimal dosage of an individual subject or groups may be determined as follows. A dose of approximately one or two grams per day is merely suggested as an illustrative starting dose. The daily dose may be increased as needed until the desired result is observed.
The intent of the invention is to not limit the dose range employed. Therefore, depending on the subject(s) the daily dose administered may approximate thirty, forty, fifty, sixty, seventy, eighty, ninety or one hundred grams per day. The safety profile of the pharmaceutical-grade ferric citrate allows the implementation of a broad range of doses.
Further, it is the intent of the invention to not be limited to capsules and tablets as oral formulations. It is known in the art that a wide variety of oral formulations may be adapted for use with the invention.
Illustrative Example of a Dosage Regimen
An non-limiting example of a dosing regimen is provided below. This is not meant to limit the invention as to how an effective amount of ferric citrate is selected, or the form in which it is provided or the frequency of administering the composition per day. The following merely illustrates how ferric citrate and placebo may be administered; e.g., as 500 mg capsules of identical appearance. All patients may receive (in a blinded fashion) 4 capsules with each of three meals, on a daily basis, for 28 days. Patients will be instructed to take the study medication within 10 minutes of finishing their meals (breakfast, lunch, and dinner).
The number of placebo, and active capsules to be taken at each meal, are as follows:
Placebo Arm of the Study
Each patient's participation in the trial lasts for up to 8 weeks: the screening period (approximately 1-2 weeks), a 1-2 week washout, and 4 weeks of treatment with study medication.
Screening Visit 1 (Study Days −30 to −15)
The following procedures will be performed at the first screening visit:
The following procedures will be performed at Study Day 14+/−1 day.
The following procedures will be performed at Study Day 28+/−1 day or on the day of early termination.
GloboMax will be the primary data management, monitoring, and coordinating center. Case report forms (CRF) will be provided for each subject. Subjects will not be identified by name or initials on CRFs. The CRF will be monitored at the clinical sites and collected by GloboMax's study monitor. Audited CRFs will be used to create electronic data files.
Three major categories of endpoints reflect biochemical and clinical issues being addressed at the outset. Additional clinical and biochemical issues are addressed as they arise. Therefore, the endpoints are not meant to limit the totality of relevant findings and measurements collected in these, or future studies.
Primary Endpoints (see
It is further noted that in comparison to chemical grade ferric citrate, the pharmaceutical grade ferric citrate demonstrates similar efficacy. See
Safety Endpoints (see
Safety will be monitored by recording adverse events (
Specific rules for withdrawal from the study, based on laboratory data, have also been set up to ensure patient safety. A nonlimiting example of such criteria is illustrated by the following:
If a patient's serum phosphate level increases to ≧10 mg/dL at any time during the study period, the patient will be withdrawn from the study.
Specific studies have also shown that pharmaceutical grade ferric citrate possesses similar efficacy to chemical grade ferric citrate. (See
Kwok, David W. K., Stoynov, Nikolay Mintchev, Chan, Keith, Town, Winston
Patent | Priority | Assignee | Title |
10300039, | Jul 21 2009 | Keryx Biopharmaceuticals, Inc. | Ferric citrate dosage forms |
11466042, | Nov 10 2017 | Tokuyama Corporation | Method for producing ferric citrate hydrate |
9889113, | Jan 30 2006 | Panion & BF Biotech Inc. | Method for reversing, preventing, delaying or stabilizing soft tissue calcification |
Patent | Priority | Assignee | Title |
3591616, | |||
4180567, | Sep 02 1977 | Pharmachem Corporation | Iron preparations and methods of making and administering the same |
4689322, | Jul 28 1982 | MEDICE CHEM PHARM FABRIK PUETTER GMBH & CO KG | Pharmaceutical products, calcium mixed salts of polymeric, anionic carboxylic acids and/or their esters of sulfuric acid, and methods for their preparation and use |
4970079, | Jun 05 1989 | Purdue Research Foundation | Method and composition of oxy-iron compounds for treatment of hyperphosphatemia |
5206265, | Sep 14 1987 | Schering Aktiengesellschaft | Iron citrate complex, process for its production, and its pharmaceutical |
5707980, | Aug 17 1990 | Bone Care International, Inc. | Method for treating and preventing secondary hyperparathyroidism |
5753706, | Feb 03 1997 | HSU, CHEN HSING | Methods for treating renal failure |
6887897, | Jul 31 2001 | Mission Pharmacal Company | Calcium glutarate supplement and phosphorus binder |
6903235, | Oct 08 2003 | Panion & BF Biotech Inc. | Pharmaceutical-grade ferric citrate |
7767851, | Feb 19 2003 | PANION & BF BIOTECH INC | Ferric organic compounds, uses thereof and methods of making same |
8093423, | Feb 19 2003 | PANION & BF BIOTECH INC | Pharmaceutical-grade ferric organic compounds, uses thereof and method of making same |
8299298, | Feb 19 2003 | PANION & BF BIOTECH INC | Pharmaceutical-grade ferric organic compounds, uses thereof and method of making same |
8754257, | Feb 19 2003 | PANION & BF BIOTECH INC | Pharmaceutical-grade ferric organic compounds, uses thereof and methods of making same |
8754258, | Feb 19 2003 | PANION & BF BIOTECH INC | Ferric organic compounds, uses thereof and methods of making same |
8846976, | Feb 19 2003 | PANION & BF BIOTECH INC | Ferric organic compounds, uses thereof and methods of making same |
9050316, | Feb 19 2003 | PANION & BF BIOTECH INC | Pharmaceutical-grade ferric organic compounds, uses thereof and methods of making same |
20050080283, | |||
20060020026, | |||
20080274210, | |||
20090186939, | |||
20090326060, | |||
20100217025, | |||
AU199854419, | |||
AU2004213819, | |||
AU2004216819, | |||
AU2006279333, | |||
AU2007210090, | |||
AU2007210096, | |||
AU723901, | |||
CA2272711, | |||
CA2516471, | |||
CA2619591, | |||
CA2640673, | |||
CA2640974, | |||
CN31574904, | |||
CN101019848, | |||
CN101235186, | |||
CN101374416, | |||
CN101378658, | |||
CN1315174, | |||
CN1446790, | |||
CN1600302, | |||
CN1751056, | |||
DE1131360, | |||
EA10028, | |||
EA20050132226, | |||
EA200800593126, | |||
EP308362, | |||
EP600347, | |||
EP959878, | |||
EP101235186, | |||
EP1601680, | |||
EP1931689, | |||
EP1978807, | |||
EP1978808, | |||
GB1224589, | |||
GB1226394, | |||
GB2212396, | |||
HK1077580, | |||
ID200502228, | |||
IL130041, | |||
IL170385, | |||
IL189583, | |||
IL192545, | |||
IL193099, | |||
IN944MUMNP2005, | |||
IN1413MUMNP2008, | |||
IN1414MUMNP2008, | |||
IN244119, | |||
IN393MUMNP20008, | |||
JP2001506262, | |||
JP2006518391, | |||
JP2007133978, | |||
JP2008552431, | |||
JP2008552435, | |||
JP200924341, | |||
JP2009504777, | |||
JP2009525276, | |||
JP4173553, | |||
JP8198760, | |||
KR1020050107428, | |||
KR1020080094013, | |||
KR1020080106506, | |||
KR10200870106131, | |||
KR464504, | |||
LK13792, | |||
MLI20063971, | |||
MX207250, | |||
MXA5008784, | |||
MXXA2008002360, | |||
NO19992936, | |||
NO327148, | |||
NZ336060, | |||
NZ541991, | |||
NZ566743, | |||
PGGP500029, | |||
PH12005501521, | |||
RU2188033, | |||
SG114272, | |||
SG2005052592, | |||
SU142643, | |||
TL61003938, | |||
TW259772, | |||
TW86104116, | |||
TW93103743, | |||
TW95130373, | |||
VN1200501292, | |||
VN8033, | |||
WO2004074444, | |||
WO2007022435, | |||
WO2007089571, | |||
WO2007089577, | |||
WO2011011541, | |||
WO9826776, |
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